DSpace at EWHA: Syndecan-2 functions as an adhesion receptor in colon cancer cells

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DSpace at EWHA일반대학원 생명·약학부 Theses_Ph.D

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DC Field	Value	Language
dc.contributor.advisor	오억수	-
dc.contributor.author	김연희	-
dc.creator	김연희	-
dc.date.accessioned	2016-08-26T04:08:22Z	-
dc.date.available	2016-08-26T04:08:22Z	-
dc.date.issued	2012	-
dc.identifier.other	OAK-000000072137	-
dc.identifier.uri	https://dspace.ewha.ac.kr/handle/2015.oak/211049	-
dc.identifier.uri	http://dcollection.ewha.ac.kr/jsp/common/DcLoOrgPer.jsp?sItemId=000000072137	-
dc.description.abstract	Syndecan-2 is one of transmembrane heparan sulfate proteoglycans that act as cell surface receptor during cell-extracellular matrix interaction. At cell adhesion sites, syndecan-2 can impact on various adhesion-related cell functions, but details of the regulatory mechanism governing syndecan-2 are not well known. Here, I examined the regulatory role of syndecan-2 as an adhesion receptor in colon cancer cells. Overexpression of syndecan-2 enhanced collagen adhesion, cell migration and invasion of normal rat intestinal epithelial cells(RIE1), and increased integrin 2 expression levels. Interestingly, RIE1 cells transfected with either syndecan-2 or integrin 2 showed similar adhesion and migration patterns, and a function-blocking anti-integrin 2 antibody abolished syndecan-2-mediated adhesion and migration. Consistent with these findings, transfection of integrin 2 siRNA diminished syndecan-2-induced cell migration in HCT116 human colon cancer cells, suggesting a novel cooperation between syndecan-2 and integrin 21 in adhesion-mediated cell migration and invasion. Interestingly, colon cancer cells transfected with various syndecan-2-encoding genes with deletions in the cytoplasmic domain showed that syndecan-2-induced migration activity requires the EFYA sequence of the C-terminal region; deletion of these residues abolished the rise in cell migration seen when the wild-type gene was transfected and syndecan-2 interaction with syntenin-1, suggesting that syntenin-1 functioned as a cytosolic signal effector downstream from syndecan-2. Colon cancer cells overexpressing the syntenin-1 gene showed increased migratory activity, whereas migration was decreased in cells in which syntenin-1 was knock-down using small inhibitory RNA. In addition, syntenin-1 expression potentiated colon cancer cell migration induced by syndecan-2, and syndecan-2-mediated cell migration was reduced when syntenin-1 expression diminished. However, syntenin-1-mediated migration enhancement was not noted in colon cancer cells transfected with a gene encoding a syndecan-2 mutant lacking the cytoplasmic domain. Furthermore, in line with the increase in cell migration, syntenin-1 mediated Rac activation stimulated by syndecan-2. Therefore, the cytoplasmic domain of syndecan-2 seems to regulate colon cancer cell migration via interaction with syntenin-1. Taken together, all these results demonstrate that syndecan-2 plays an important role as an adhesion receptor regulating adhesion-mediated functions in colon cancer cells. This interactive dynamics between syndecan-2 and other cell surface receptor (e.g. integrin α2β1) and/or cytosolic effector (e.g. syntenin-1) might be a possible mechanism underlying the tumorigenic activities of colon cancer cells.;Ttransmembrane heparin sulfate proteoglycan 인 Syndecan 은 adhesion receptor 로서 세포부착과 이동에 관여를 하고 있으나, 그 세부적인 기작에 대해서 아직도 많은 연구가 수행되고 있다. 본 연구에서는 Syndecan-2 의 adhesion receptor, 세포질내의 interaction, oligomerization 등을 통한 대장암세포에서의 세포 이동에 대한 영향을 알아보고자 하였다. Nomal rat intestinal epithelial cells(RIEI)에 syndecan-2 를 과발현 시켰을 때, 대표적인 cell adhesion receptor 인 integrin α2 의 발현이 증가함을 확인할 수 있었다. 또한 syndecan과 integrin α2 의 발현을 각각 증가시켰을 때, 모두 cell migration이 증가함을 확인할 수 있었으며, 놀랍게도 integrin α2 를 억제시켰을 때, syndecan-2 에 의해 유도되는 cell adhesion 과 migration 이 감소됨을 알 수 있었다. 이러한 것은 syndecan-2 의 발현을 억제하였을 때도 같은 결과를 얻었다. 이러한 syndecan-2 와 integrin α2와의 관계가 RIEI cells 에서 뿐 만이 아니라, colon cancer cells 에서도 동일함을 확인할 수 있었다. Syndecan 은 세포질내에서 다양한 단백질들과 결합하여, 세포부착 및 이동 등 다양한 역할을 수행하고 있다. 이러한 세포질 내에서의 기능을 알아보기 위하여 syndecan-2 의 다양한 construct를 발현시키고, 이미 syndecan-2 와 결합한다고 알려진 syntenin 과의 결합이 cell migration 에 어떤 영향을 주는지 알아보았다. Syntenin 과 syndecan-2 cytoplasmic domain 의 결합으로 cell migration이 증가하고 그 downstream 인 Rac 이 activation 됨을 확인할 수 있었다. Syndecan 을 포함한 receptor 들은 대부분 dimerization 등을 통하여 활성화기작이 유도된다. Syndecan 의 경우, non-covalent dimerization 이 유도됨이 알려져 있다. 본 연구에서는 fibronectin matrix 하에서 syndecan 을 과발현 시켰을 때, cell spreading 및 migration 이 증가함을 확인하였고, 이러한 증가에 transmembrane에 의해 유도된 dimerization 이 중요함을 확인할 수 있었다. 이러한 모든 결과를 통해 syndecan-2 가 integrin α2 의 coreceptor로서 작용을 하며, syndecan-2 의 cytoplasmic domain 과 syntenin 의 결합 및 oligomerization 이 cell migration 증가에 영향을 줌을 알 수 있었다.	-
dc.description.tableofcontents	INTRODUCTION 1 Structure of syndecans 1 Syndecans and cancer 4 Functions of syndecans 6 Roles of syndecan-2 as an adhesion receptor 6 Integrins 8 Binding of partners of syndecan-2 cytoplasmic domian 9 Syntenin 12 Oligomerization of syndecans 12 The goals of the thesis 14 CHAPTER I 15 1. INTRODUCTION 16 2. MATERIAL & METHODS 18 2-1. Reagents and antibodies 18 2-2. Cell culture and transfection 18 2-3. Fluorescence-activated cell sorting(FACS) analysis 19 2-4. Proliferation assay 20 2-5. Cell adhesion assay 20 2-6. Wound-closure, cell migration and invasion assays 21 2-7. Immunoblotting 22 2-8. Synthesis of small interfering RNA(siRNA) construct 22 2-9. RNA extraction and reverse transfection polymerase chain reaction (RT-PCR) 23 3. RESULTS 25 3-1. Syndecan-2 expression enhances adhesion on collagen and migration of RIE1 cells 25 3-2. Syndecan-2-mediated adhesion and migration are dependent on integrin a2 29 3-3. Increased syndecan-2 cooperatively regulates cell migration with integrin a2 in HCT116 human colon carcinoma cells 35 CHAPTER II 38 1. INTRODUCTION 39 2. MATERIAL & METHODS 42 2-1. Reagents and antibodies 42 2-2. Cell culture and transfection 42 2-3. Molecular construct 43 2-4. Synthesis and transfection of siRNA constructs 44 2-5. RNA extraction and reverse transfection polymerase chain reaction (RT-PCR) 44 2-6. Immunoblotting 45 2-7. Transwell migration assay 46 2-8. GST-pull down assays 46 2-9. GST-PAK-PBD binding assay 47 3. RESULTS 48 3-1. Syndecan-2 cytoplasmic domain is involved in regulation of cell migtation 48 3-2. Syntenin-1 regulates colon cancer cell migration 52 3-3. Syntenin-1 regulates syndecan-2-mediated colon cancer cell migration 56 CHAPTER III 61 1. INTRODUCTION 62 2. MATERIAL & METHODS 64 2-1. Cell culture, antibodies and reagents 64 2-2. RNA extraction and reverse transcription polymerase chain reaction(RT-PCR) 64 2-3. Fluorescence-activated cell sorting (FACS) analysis 65 2-4. Cell spreading assay 65 2-5. Monitoring cell spreading 66 2-6. Centrifugal detachment assay 66 2-7. Transwell migration assay 67 2-8. Wound healing assay 67 2-9. Synthesis of small interfering RNA (siRNA) constructs 68 2-10. Protrusive force measuring 68 3. RESULTS 70 3-1. Syndecan-2 overexpression induces cell attachment and spreading on fibronection matrix 70 3-2. Syndecan-2 expression is correlated with the enhanced ECM interaction 73 3-3. Abolishment of syndecan-2 dimerization through transmembrane domain affects spreading and migration on fibronectin matrix 75 3-4. Syndecan-2 dimerization through transmembrane domain enhances attachment and cell-ECM interaction 78 DISCUSSION 81 A. Serve as cell surface co-receptor 82 B. Role of scaffolding proteins 85 C. Trnasmembrane domain-mediated oligomerization 88 D. Conclusion 91 REFERENCES 93 논문개요 108 ACKNOWLEDGEMENT 110 PUBLICATION LISTS 114	-
dc.format	application/pdf	-
dc.format.extent	4966395 bytes	-
dc.language	eng	-
dc.publisher	이화여자대학교 대학원	-
dc.subject.ddc	600	-
dc.title	Syndecan-2 functions as an adhesion receptor in colon cancer cells	-
dc.type	Doctoral Thesis	-
dc.format.page	xii, 115 p.	-
dc.identifier.thesisdegree	Doctor	-
dc.identifier.major	대학원 생명·약학부생명과학전공	-
dc.date.awarded	2012. 8	-